Isoxazolidine-acids

Isoxazoles, isoxazolines, isoxazolidines and benzisoxazoles are all thermally stable, distilling without decomposition, but the stability of the system depends on the substitution pattern. For example, aminoisoxazoles distill unchanged but the isoxazole carboxylic acids usually decompose at or above their melting points without giving the corresponding isoxazole. 

Oxidation of fused isoxazolidine (173) with one equivalent of m-chloroperbenzoic acid produced an oxazine. The mechanism of transformation involves formation of an A/-oxide... 

In general,. alkoxy- or silyloxy-isoxazolidines when treated with acid produce 2-isoxazo-lines <77AHC(2i)207, 74MIP41601). Other isoxazolidines are cleaved at the N—O bond with further degradation then following <77AHC(2i)207). The treatment of (182) with HCl generated cinnamic acid and a small amount of benzoic acid, whereas treatment of (182) with... 

Isoxazolidine reacted with acetone and perchloric acid to produce the iminium salt (189) <80JA1649). 

Nitrones or aci-nitro esters react with alkenes to give in some cases A/-substituted isoxazolidines and in others 2-isoxazolines. When the intermediate isoxazolidines were observed, a number of procedures transformed them into the 2-isoxazolines. Acrylonitrile and phenyl rzcf-nitrone esters produced an A/-methoxyisoxazolidine. Treatment with acid generated a 2-isoxazole while treatment with base generated an oxazine (Scheme 118) (68ZOR236). When an ethoxycarbonyl nitrone ester was reacted with alkenes, no intermediate isoxazolidine was observed, only A -isoxazolines. Other aci-mtro methyl esters used are shown in Scheme 118 and these generate IV-methoxyisoxazolidines or A -isoxazolines which can be further transformed (72MI41605). 

Treatment of (537) with acid chloride (538) in the presence of triethylamine produced isoxazolidine (539) in 45% yield (80IZV1694). 

Isoxazolidine, 2-(trimethyIsiIyloxy)-5-methoxycarbonyl-reactions with acids, 6, 47... 

IsoxazoIidine-3,3-dicarboxylic acid, 2-methoxy-dimethyl ester reaction with bases, 6, 47 Isoxazolidine-3,5-diones synthesis, 6, 112, 113 Isoxazoli dines conformation, 6, 10 3,5-disubstituted synthesis, 6, 109 oxidation, 6, 45-46 PE spectra, 6, 5 photolysis, 6, 46 pyrolysis, 6, 46 reactions, 6, 45-47 with acetone, 6, 47 with bases, 6, 47 reduction, 6, 45 ring fission, S, 80 spectroscopy, 6, 6 synthesis, 6, 3, 108-112 thermochemistry, 6, 10 Isoxazolidin-3-ol synthesis, 6, 111 Isoxazolidin-5-oI synthesis, 6, 111... 

Nitronates derived from primary nitroalkanes can be regarded as a synthetic equivalent of nitrile oxides since the elimination of an alcohol molecule from nitronates adds one higher oxidation level leading to nitrile oxides. This direct / -elimination of nitronates is known to be facilitated in the presence of a Lewis acid or a base catalyst [66, 72, 73]. On the other hand, cycloaddition reactions of nitronates to alkene dipolarophiles produce N-alkoxy-substituted isoxazolidines as cycloadducts. Under acid-catalyzed conditions, these isoxazolidines can be transformed into 2-isoxazolines through a ready / -elimination, and 2-isoxazolines correspond to the cycloadducts of nitrile oxide cycloadditions to alkenes [74]. 

Because of the relative instabihty of many trimethylsilyl nitronates 1036, 1037, they should be reacted in situ with olefins 1053 [103-105] or acetylenes [127] to generate the isooxazolidines 1054 [103-105, 107-117, 119-133] or isoxazoles [127] (Scheme 7.37) The isoxazolidines 1054 with R2=H readily ehminate trimethylsilanol 4 in the presence of acids such as TsOH to form the isoxazolines 1055 in high yields [104, 105] (Scheme 7.37 cf. also the cycloadditions with acrylonitrile in Scheme 7.42). 

Asymmetric 1,3-dipolar cycloaddition of cyclic nitrones to crotonic acid derivatives bearing chiral auxiliaries in the presence of zinc iodide gives bicyclic isoxazolidines with high stereoselectivity (Eq. 8.51). The products are good precursors of (3-amino acids such as (+)sedridine.73 Many papers concerning 1,3-dipolar cycloaddition of nitrones to chiral alkenes have been reported, and they are well documented (see Ref. 63). 

A-Unsubstituted isoxazolidines such as 65 undergo facile decarboxylative peptide couplings with a-keto acids <06JA1452>. The use of water as solvent or cosolvent was particularly beneficial for the formation of amides in high yields. The methyl a-keto esters obtained could be saponified to the corresponding a-keto acids, and the (i-peptide chain could then be extended by reaction with another isoxazolidine. 

Nitrone 1,3-DC reactions are still the most general approach to isoxazolidines. The stereocontrol is usually achieved by the use of chiral nitrones and/or dipolarophiles, but new interesting achievements on Lewis acid catalyzed cycloadditions are also frequently reported. Tris(6,6,7,7,8,8,8-heptafluoro-2,2-dimethyl-3,5-octanatedionate) europium(III) [Eu(fod)3] selectively activated the Z-isomer of C-alkoxycarbonyl nitrone 75 existing as an E,Z-equilibrium mixture by forming the (Z)-75-Eu(fod)3 complex. (Z)-75-Eu(fod)3 reacted with electron-rich dipolarophiles such as vinyl ethers to give the trans-adducts with excellent diastereoselectivity <06T12227>. 

Bis(oxazolinyl)pyridine-Ce(IV) triflate complex 78 catalyzed the enantioselective 1,3-DC of acyclic nitrones with a, 3-unsaturated 2-acyl imidazoles. For example, C-phenyl 7V-benzyl nitrone reacted with 77 in the presence of 78 to give the adduct 79 with excellent diastereo-and enantioselectivity. Isoxazolidine 79 was then converted into P -hydroxy-P-amino acid derivatives by hydrogenation of the N-0 bond in the presence of Pd(OH)2/C and cleavage of the 2-acyl imidazole with MeOTf in MeCN <06OL3351>. 

Spirocyclopropane isoxazolidines 75, obtained from alkylidenecyclopropane nitrones, underwent thermally induced selective rearrangement to pyrrolo[3,4-A]pyridinones 76 <00TA897>. The same adducts 75 in the presence of a protic acid afforded exclusively p-lactams 77 (57-60% yield) accompanied by ethylene extrusion <00JA8075>. 

The optically active isoxazolidines obtained in these cycloaddition reactions can be easily transformed into biologically active 3 -amino acids, into j3-lactams and into important chiral building blocks such as y-amino alcohols. The multitude of synthetic results in these reactions is of course expected by the wide variety... 

Isoxazolidine cycloadducts (491) undergo easy transformation into a-amino-y-lactones (494), which can be readily converted into y- hydroxy-a-amino acids (495) (Scheme 2.240) (Table 2.19). 

Dipolar cycloaddition reactions between three A-benzyl-C-glycosyl nitrones and methyl acrylate afforded key intermediates for the synthesis of glyco-syl pyrrolidines. It was found that furanosyl nitrones (574) and (575) reacted with methyl acrylate to give mixtures of all possible 3,5-disubstituted isoxazolidines (577) and (578). On the other hand, the reaction with pyranosyl nitrone (576) was much more selective and cycloaddition at ambient temperatures afforded only one of the possible Re-endo adducts (579a). The obtained isoxazolidines were transformed into the corresponding (V-benzyl-3-hydroxy-2-pyrrolidinones (580—582) on treatment with Zn in acetic acid (Scheme 2.264) (773). 

The 1,3-dipolar cycloaddition of nitrones to vinyl ethers is accelerated by Ti(IV) species. The efficiency of the catalyst depends on its complexation capacity. The use of Ti( PrO)2Cl2 favors the formation of trans cycloadducts, presumably, via an endo bidentate complex, in which the metal atom is simultaneously coordinated to the vinyl ether and to the cyclic nitrone or to the Z-isomer of the acyclic nitrones (800a). Highly diastereo- and enantioselective 1,3-dipolar cycloaddition reactions of nitrones with alkenes, catalyzed by chiral polybi-naphtyl Lewis acids, have been developed. Isoxazolidines with up to 99% ee were obtained. The chiral polymer ligand influences the stereoselectivity to the same extent as its monomeric version, but has the advantage of easy recovery and reuse (800b). 

At the same time, the reactions of isoxazolidines (239) with soft acids and retain LA (157, 341, 398, 399) resemble an analogous process considered above for iV-siloxynitroso acetals, which also affords isoxazolines (240). Methanol can be eliminated from nitroso acetals (239) also upon heating (341). 

Conversion of isoxazolidines to the corresponding /V-methyl 7-aminoalcohols was achieved by methylation with Mel followed by reduction with Zn in acetic acid or hydrogenation over Pd/C (Equation 25) <1997TA293>. 

In 2002, Kiindig et al. [23, 24] developed catalytic DCR between diaryl nitrones and a,(3-unsaturated aldehydes in the presence of Binop-F iron and ruthenium complexes as chiral Lewis-acid catalysts (Scheme 6). The corresponding cycloadducts were obtained in good yields with complete endo selectivity and up to 94% ee. The isoxazolidine products were obtained as a mixture of regioi-somers in molar ratios varying from 96 4 to 15 85. Experimental and computational data show that the regioselectivity correlates directly with the electronic properties of the nitrone. 

Cycloaddition of nitrones (e.g. 166, equation 107) to alkoxyaUtenes proceeds in high yield with complete diastereoselectivity, giving 1,2-isoxazolidines of type 167. Similar reactions have been reported for vinyl ethers , vinyl acetate , enamines , vinyl imidazoles , enamides, vinyl sulfones and vinyl sulfides . Since the resultant 1,2-oxazolidines of type 167 and its analogs can be hydrolyzed under acidic conditions, this reaction may also be considered as an approach to O-unsubstituted N-alkylhydroxylamines . 

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